Your search keyword '"Zun‐Fu Ke"' showing total 6 results

1. Methylation of N6 adenosine‐related long noncoding RNA: effects on prognosis and treatment in ‘driver‐gene‐negative’ lung adenocarcinoma

Author

Hao‐Shuai Yang, He‐Yuan Cai, Shi‐Chao Shan, Ting‐Fei Chen, Jian‐Yong Zou, Maimaiti Abudurufu, Hong‐He Luo, Yi‐Yan Lei, Zun‐Fu Ke, and Ying Zhu

Subjects

driver‐gene‐negative, long noncoding RNA, lung adenocarcinoma, N6 adenosine methylation, nomogram, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The improvement of treatment for patients with ‘driver‐gene‐negative’ lung adenocarcinoma (LUAD) remains a critical problem to be solved. We aimed to explore the role of methylation of N6 adenosine (m6A)‐related long noncoding RNA (lncRNA) in stratifying ‘driver‐gene‐negative’ LUAD risk. Patients negative for mutations in EGFR, KRAS, BRAF, HER2, MET, ALK, RET, and ROS1 were identified as ‘driver‐gene‐negative’ cases. RNA sequencing was performed in 46 paired tumors and adjacent normal tissues from patients with ‘driver‐gene‐negative’ LUAD. Twenty‐three m6A regulators and relevant lncRNAs were identified using Pearson's correlation analysis. K‐means cluster analysis was used to stratify patients, and a prognostic nomogram was developed. The CIBERSORT and pRRophetic algorithms were employed to quantify the immune microenvironment and chemosensitivity. We identified two clusters highly consistent with the prognosis based on their unique expression profiles for 46 m6AlncRNAs. A risk model constructed from nine m6A lncRNAs could stratify patients into high‐ and low‐risk groups with promising predictive power (C‐index = 0.824), and the risk score was an independent prognostic factor. The clusters and risk models were closely related to immune characteristics and chemosensitivity. Additional pan‐cancer analysis using the nine m6AlncRNAs showed that the expression of DIO3 opposite strand upstream RNA (DIO3OS) is closely related to the immune/stromal score and tumor stemness in a variety of cancers. Our results show that m6AlncRNAs are a reliable prognostic tool and can aid treatment decision‐making in ‘driver‐gene‐negative’ LUAD. DIO3OS is associated with the development of various cancers and has potential clinical applications.

Published

2023

2. Methylation of <scp>N6</scp> adenosine‐related long noncoding <scp>RNA</scp> : effects on prognosis and treatment in ‘driver‐gene‐negative’ lung adenocarcinoma

Author

Hao‐Shuai Yang, He‐Yuan Cai, Shi‐Chao Shan, Ting‐Fei Chen, Jian‐Yong Zou, Maimaiti Abudurufu, Hong‐He Luo, Yi‐Yan Lei, Zun‐Fu Ke, and Ying Zhu

Subjects

Cancer Research, Oncology, Genetics, Molecular Medicine, General Medicine

Abstract

The improvement of treatment for patients with 'driver-gene-negative' lung adenocarcinoma (LUAD) remains a critical problem to be solved. We aimed to explore the role of methylation of N6 adenosine (m6A)-related long noncoding RNA (lncRNA) in stratifying 'driver-gene-negative' LUAD risk. Patients negative for mutations in EGFR, KRAS, BRAF, HER2, MET, ALK, RET, and ROS1 were identified as 'driver-gene-negative' cases. RNA sequencing was performed in 46 paired tumors and adjacent normal tissues from patients with 'driver-gene-negative' LUAD. Twenty-three m6A regulators and relevant lncRNAs were identified using Pearson's correlation analysis. K-means cluster analysis was used to stratify patients, and a prognostic nomogram was developed. The CIBERSORT and pRRophetic algorithms were employed to quantify the immune microenvironment and chemosensitivity. We identified two clusters highly consistent with the prognosis based on their unique expression profiles for 46 m6AlncRNAs. A risk model constructed from nine m6A lncRNAs could stratify patients into high- and low-risk groups with promising predictive power (C-index = 0.824), and the risk score was an independent prognostic factor. The clusters and risk models were closely related to immune characteristics and chemosensitivity. Additional pan-cancer analysis using the nine m6AlncRNAs showed that the expression of DIO3 opposite strand upstream RNA (DIO3OS) is closely related to the immune/stromal score and tumor stemness in a variety of cancers. Our results show that m6AlncRNAs are a reliable prognostic tool and can aid treatment decision-making in 'driver-gene-negative' LUAD. DIO3OS is associated with the development of various cancers and has potential clinical applications.

Published

2022

3. A radiomics nomogram prediction for survival of patients with 'driver gene-negative' lung adenocarcinomas (LUAD)

Author

Qi-Kun Guo, Hao-Shuai Yang, Shi-Chao Shan, Dan-Dan Chang, Li-Jie Qiu, Hong-He Luo, He-Ping Li, Zun-Fu Ke, and Ying Zhu

Subjects

Radiology, Nuclear Medicine and imaging, General Medicine

Abstract

Background To study the role of computed tomography (CT)-derived radiomics features and clinical characteristics on the prognosis of “driver gene-negative” lung adenocarcinoma (LUAD) and to explore the potential molecular biological which may be helpful for patients’ individual postoperative care. Methods A total of 180 patients with stage I-III “driver gene-negative” LUAD in the First Affiliated Hospital of Sun Yat-Sen University from September 2003 to June 2015 were retrospectively collected. The Least Absolute Shrinkage and Selection Operator (LASSO) Cox regression model was used to screen radiomics features and calculated the Rad-score. The prediction performance of the nomogram model based on radiomics features and clinical characteristics was validated and then assessed with respect to calibration. Gene set enrichment analysis (GSEA) was used to explore the relevant biological pathways. Results The radiomics and the clinicopathological characteristics were combined to construct a nomogram resulted in better performance for the estimation of OS (C-index: 0.815; 95% confidence interval [CI]: 0.756–0.874) than the clinicopathological nomogram (C-index: 0.765; 95% CI: 0.692–0.837). Decision curve analysis demonstrated that in terms of clinical usefulness, the radiomics nomogram outperformed the traditional staging system and the clinicopathological nomogram. The clinical prognostic risk score of each patient was calculated based on the radiomics nomogram and divided by X-tile into high-risk (> 65.28) and low-risk (≤ 65.28) groups. GSEA results showed that the low-risk score group was directly related to amino acid metabolism, and the high-risk score group was related to immune and metabolism pathways. Conclusions The radiomics nomogram was promising to predict the prognosis of patients with “driver gene-negative” LUAD. The metabolism and immune-related pathways may provide new treatment orientation for this genetically unique subset of patients, which may serve as a potential tool to guide individual postoperative care for those patients.

Published

2023

4. Author response for 'Methylation of <scp>N6</scp> adenosine‐related long non‐coding <scp>RNA</scp> : effects on prognosis and treatment in 'driver‐gene‐negative' lung adenocarcinoma'

Author

null Hao‐Shuai Yang, null He‐Yuan Cai, null Shi‐Chao Shan, null Ting‐Fei Chen, null Jian‐Yong Zou, null Maimaiti Abudurufu, null Hong‐He Luo, null Yi‐Yan Lei, null Zun‐Fu Ke, and null Ying Zhu

Published

2022

5. Circulating Tumor Cells for Stratification of Recurrence Risk in Stage II Colorectal Cancer: A Multicenter Cohort Study

Author

Wenpeng Zhou, Lili Chen, Ziyin Ye, Xiaoming Zhong, Jianwen Zhou, Shaohong Chen, Wei Liu, Yu Sun, Lijuan Ren, Xiaojun Tan, Zhirong Zeng, Ji Cui, Weiling He, and Zun-Fu Ke

Published

2022

6. Exploration of the Effects of Methylation of N6 Adenosine (m6A) Related lncRNA on Prognosis and Treatment in 'Driver-Gene-Negative' Lung Adenocarcinoma (LUAD)

Author

Hao-Shuai Yang, He-Yuan Cai, Shi-Chao Shan, Ting-Fei Chen, Jian-Yong Zou, Hong-He Luo, Yi-Yan Lei, Zun-Fu Ke, and Ying Zhu

Published

2022